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采用外翻肠囊法研究聚普瑞锌(L-肌肽锌络合物)的吸收机制。

Absorption mechanism of polaprezinc (zinc L-carnosine complex) by an everted sac method.

作者信息

Furuta S, Toyama S, Sano H

机构信息

Central Research Laboratories, Zeria Pharmaceutical Co. Ltd., Saitama, Japan.

出版信息

Xenobiotica. 1994 Nov;24(11):1085-94. doi: 10.3109/00498259409038668.

DOI:10.3109/00498259409038668
PMID:7701850
Abstract
  1. The absorption mechanism of polaprezinc (zinc-carnosine chelate compound) was studied in rat by an everted gut sac method. The rates of transport and accumulation of 14C-L-carnosine were proportional to the mucosal concentration of L-carnosine, whereas the rates of transport and accumulation of 65ZnCl2 had become saturated. The Michaelis-Menten constant (Km) = 4.41 mM and maximal rate (Vmax) = 71.83 nmol/min/g for zinc transport and, similarly, Km = 6.21 mM and Vmax = 92.51 mumol/30 min/g for accumulation. 2. The addition of ouabain, 2,4-dinitrophenol (2,4-DNP) and low temperatures reduced the rate of zinc uptake, indicating that zinc transport was considered to be a carrier-mediated process based on Na+,K(+)-ATPase-dependent mechanisms. 3. The concentration of zinc in the gut of the non-fasted rat was greater than that of the fasted rat, suggesting different rates of transport and accumulation. It is suggested that zinc intestinal uptake in rat is regulated by zinc content in the gut. 4. A pharmacokinetic model for transport and accumulation of zinc saturation from the lumen side to the gut was designed, and the calculated values obtained by simultaneous multiline fitting of transport and accumulation of zinc data were in good agreement with the observed values.
摘要
  1. 采用外翻肠囊法在大鼠体内研究了聚普瑞锌(锌 - 肌肽螯合物)的吸收机制。14C - L - 肌肽的转运和积累速率与L - 肌肽的黏膜浓度成正比,而65ZnCl2的转运和积累速率已达到饱和。锌转运的米氏常数(Km)= 4.41 mM,最大速率(Vmax)= 71.83 nmol/min/g;同样,积累的Km = 6.21 mM,Vmax = 92.51 μmol/30 min/g。2. 加入哇巴因、2,4 - 二硝基苯酚(2,4 - DNP)和降低温度会降低锌的摄取速率,这表明锌的转运被认为是基于Na +,K(+) - ATP酶依赖性机制的载体介导过程。3. 非禁食大鼠肠道中的锌浓度高于禁食大鼠,表明转运和积累速率不同。提示大鼠肠道对锌的摄取受肠道中锌含量的调节。4. 设计了一个从肠腔侧到肠道的锌饱和转运和积累的药代动力学模型,通过对锌数据的转运和积累进行同步多线拟合得到的计算值与观测值吻合良好。

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1
Absorption mechanism of polaprezinc (zinc L-carnosine complex) by an everted sac method.采用外翻肠囊法研究聚普瑞锌(L-肌肽锌络合物)的吸收机制。
Xenobiotica. 1994 Nov;24(11):1085-94. doi: 10.3109/00498259409038668.
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Jpn J Pharmacol. 1995 Apr;67(4):271-8. doi: 10.1254/jjp.67.271.
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J Pharm Biomed Anal. 1999 Mar;19(3-4):453-61. doi: 10.1016/s0731-7085(98)00236-2.
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A comparison of the cellular actions of polaprezinc (zinc-L-carnosine) and ZnCl2.聚甘醇锌(L-肉碱锌)和氯化锌的细胞作用比较。
Life Sci. 2012 Jun 27;90(25-26):1015-9. doi: 10.1016/j.lfs.2012.05.017. Epub 2012 Jun 5.
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Polaprezinc, a zinc compound, is distributed to the lingual epithelium and increases its zinc concentration in zinc-deficient rats.聚普瑞锌,一种锌化合物,在缺锌大鼠体内可分布至舌上皮并提高其锌浓度。
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[The inhibitory effect and the mechanism of ethanol absorption by L-carnosine zinc complex in mouse gastrointestinal tract].L-肌肽锌络合物对小鼠胃肠道乙醇吸收的抑制作用及其机制
Nihon Arukoru Yakubutsu Igakkai Zasshi. 1998 Dec;33(6):692-702.
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Polaprezinc prevents ongoing thioacetamide-induced liver fibrosis in rats.波拉普利锌可预防噻唑烷二酮诱导的大鼠肝纤维化。
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Preventive effect of zinc compounds, polaprezinc and zinc acetate against the onset of hepatitis in Long-Evans Cinnamon rat.锌化合物、聚普瑞锌和乙酸锌对长 Evans 肉桂大鼠肝炎发病的预防作用
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[Development of polaprezinc research].[聚普瑞锌的研究进展]
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